Figure 4
Figure 4. Haploid loss of ID4 in Eμ-TCL1-tg mice leads to accelerated CLL disease progression. (A) ID4 protein expression in CD19+-selected B cells from Eμ-TCL1-tg mice without (+/+) or with (+/−) haploid loss of ID4. Numbers at the bottom give the relative amounts of ID4 protein. (B) Left: WBC counts from blood smears obtained from mice aged from 2 to 8 months. Right: 100 μL of peripheral blood lymphocytes (PBL) were collected each month and measured by flow cytometry for the percentage of CD19+CD5+ cells in mice aged from 9 to 13 months. Bottom: Number of live animals from each group that was available and analyzed. *Indicates statistically significant differences based on 2-sample t tests. (C) Representative blood smear stained with Wright-Giemsa showing an increased number of circulating lymphocytes in Eμ-TCL1-tg mice with haploid loss of ID4 (age, 14 months), but not in age-matched control heterozygous ID4 mice. (D) Kaplan-Meier survival curves from F1 littermates of Eμ-TCL1-tg mice with or without the haploid loss of ID4. (E) Histologic immunophenotyping of spleen, liver, and brain from Eμ-TCL1 mice with haploid loss of ID4. Top: Obliterative lymphoma is present in the periarteriolar lymphoid sheaths (white pulp) of spleen. Middle: Evidence of lymphocyte infiltration is suggested in approximately 25% of the liver sections by intrasinusoidal neoplastic cells. Bottom: Marked hippocampal neuronal necrosis was observed in the section from brain, as well as moderate multifocal cerebral, cerebellar, and meningeal hemorrhage, indicating the infiltration of malignant lymphocytes in the brain.

Haploid loss of ID4 in Eμ-TCL1-tg mice leads to accelerated CLL disease progression. (A) ID4 protein expression in CD19+-selected B cells from Eμ-TCL1-tg mice without (+/+) or with (+/−) haploid loss of ID4. Numbers at the bottom give the relative amounts of ID4 protein. (B) Left: WBC counts from blood smears obtained from mice aged from 2 to 8 months. Right: 100 μL of peripheral blood lymphocytes (PBL) were collected each month and measured by flow cytometry for the percentage of CD19+CD5+ cells in mice aged from 9 to 13 months. Bottom: Number of live animals from each group that was available and analyzed. *Indicates statistically significant differences based on 2-sample t tests. (C) Representative blood smear stained with Wright-Giemsa showing an increased number of circulating lymphocytes in Eμ-TCL1-tg mice with haploid loss of ID4 (age, 14 months), but not in age-matched control heterozygous ID4 mice. (D) Kaplan-Meier survival curves from F1 littermates of Eμ-TCL1-tg mice with or without the haploid loss of ID4. (E) Histologic immunophenotyping of spleen, liver, and brain from Eμ-TCL1 mice with haploid loss of ID4. Top: Obliterative lymphoma is present in the periarteriolar lymphoid sheaths (white pulp) of spleen. Middle: Evidence of lymphocyte infiltration is suggested in approximately 25% of the liver sections by intrasinusoidal neoplastic cells. Bottom: Marked hippocampal neuronal necrosis was observed in the section from brain, as well as moderate multifocal cerebral, cerebellar, and meningeal hemorrhage, indicating the infiltration of malignant lymphocytes in the brain.

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